vida: extract claims from 2026-05-03-glp1-addiction-scope-oud-nicotine-cocaine-synthesis
Some checks failed
Mirror PR to Forgejo / mirror (pull_request) Has been cancelled
Some checks failed
Mirror PR to Forgejo / mirror (pull_request) Has been cancelled
- Source: inbox/queue/2026-05-03-glp1-addiction-scope-oud-nicotine-cocaine-synthesis.md - Domain: health - Claims: 0, Entities: 1 - Enrichments: 3 - Extracted by: pipeline ingest (OpenRouter anthropic/claude-sonnet-4.5) Pentagon-Agent: Vida <PIPELINE>
This commit is contained in:
Teleo Agents
parent
84206b838d
commit
a6ac1c4b4e
4 changed files with 53 additions and 2 deletions
|
|
@ -81,3 +81,10 @@ Concurrent psychotropic medication use (antidepressants, benzodiazepines) shows
|
|||
**Source:** The Lancet 2026, EVOKE/EVOKE+ Phase 3 failure
|
||||
|
||||
EVOKE/EVOKE+ Alzheimer's failure provides critical boundary evidence for GLP-1 CNS mechanism specificity. Semaglutide succeeds in addiction (VTA dopamine reward circuits) but fails in neurodegeneration (amyloid/tau pathways), demonstrating that GLP-1 receptor activation produces pathway-specific effects rather than broad neuroprotection. This supports the mesolimbic dopamine mechanism for addiction while ruling out generalized CNS benefit claims.
|
||||
|
||||
|
||||
## Extending Evidence
|
||||
|
||||
**Source:** NBC News/Pharmacy Times synthesis, April 2026
|
||||
|
||||
NBC News synthesis documents GLP-1 evidence across four substance use disorder categories: (1) OUD: liraglutide shows ~40% craving reduction in Phase 2 RCT, semaglutide reduces overdose risk in T2D+OUD comorbid population; (2) Nicotine: exenatide+NRT increases 6-week abstinence, but long-term findings mixed; (3) Cocaine/stimulants: preclinical only (liraglutide reduces methamphetamine intake in rats); (4) Population-level: GLP-1 users with pre-existing SUD show fewer ER visits, hospitalizations, deaths across substance categories (observational data with selection bias concerns). Evidence strength hierarchy: AUD > OUD > nicotine > cocaine. As of April 2026, 33 clinical trials active (15 AUD, 9 nicotine, 4 OUD, 4 cocaine). Critical limitation: all human evidence from patients with comorbid metabolic disease—efficacy without T2D/obesity comorbidity unknown.
|
||||
|
|
|
|||
|
|
@ -11,7 +11,7 @@ sourced_from: health/2026-04-24-hendershot-jama-psychiatry-semaglutide-aud-rct.m
|
|||
scope: causal
|
||||
sourcer: Hendershot CS et al.
|
||||
supports: ["glp1-receptor-agonists-address-substance-use-disorders-through-mesolimbic-dopamine-modulation", "behavioral-biological-health-dichotomy-false-for-reward-dysregulation-conditions"]
|
||||
related: ["hedonic-eating-dopamine-circuit-adapts-to-glp1-suppression-explaining-continuous-delivery-requirement", "glp1-receptor-agonists-address-substance-use-disorders-through-mesolimbic-dopamine-modulation", "behavioral-biological-health-dichotomy-false-for-reward-dysregulation-conditions", "real-world-semaglutide-shows-stronger-mace-reduction-than-select-trial", "semaglutide-produces-large-effect-aud-reduction-through-vta-dopamine-suppression"]
|
||||
related: ["hedonic-eating-dopamine-circuit-adapts-to-glp1-suppression-explaining-continuous-delivery-requirement", "glp1-receptor-agonists-address-substance-use-disorders-through-mesolimbic-dopamine-modulation", "behavioral-biological-health-dichotomy-false-for-reward-dysregulation-conditions", "real-world-semaglutide-shows-stronger-mace-reduction-than-select-trial", "semaglutide-produces-large-effect-aud-reduction-through-vta-dopamine-suppression", "glp1-receptor-agonists-demonstrate-superior-efficacy-for-alcohol-use-disorder-in-comorbid-obesity-population"]
|
||||
---
|
||||
|
||||
# Semaglutide produces large-effect-size reductions in alcohol consumption and craving through VTA dopamine reward circuit suppression
|
||||
|
|
@ -31,3 +31,10 @@ Meta-analysis confirms semaglutide as best-performing agent for alcohol reductio
|
|||
**Source:** Qeadan F et al., Addiction 2025
|
||||
|
||||
Real-world observational data from 817,309 AUD patients (5,621 with GLP-1 RA) shows 50% lower alcohol intoxication rates (IRR 0.50, 95% CI 0.40-0.63) over 24 months, consistent with Hendershot RCT findings. Effect maintained across T2DM (IRR 0.51), obesity (IRR 0.58), and combined conditions (IRR 0.58) subgroups. Provides population-scale corroboration of the VTA dopamine mechanism hypothesis, though observational confounding limits causal inference.
|
||||
|
||||
|
||||
## Extending Evidence
|
||||
|
||||
**Source:** NBC News synthesis + Session 22 Science 2025
|
||||
|
||||
The VTA dopamine mechanism is shared across all substance use disorders, not AUD-specific. GLP-1 receptors in ventral tegmental area and nucleus accumbens reduce dopamine surge from substance exposure, attenuating reward salience. This explains why GLP-1 effects extend beyond alcohol to opioids, nicotine, and potentially cocaine. However, Session 22 Science 2025 paper showed VTA dopamine circuits adapt during repeat GLP-1 treatment (mice recover hedonic eating), suggesting efficacy may fade with long-term use for some reward circuits.
|
||||
|
|
|
|||
34
entities/health/nct04199728-glp1-oud.md
Normal file
34
entities/health/nct04199728-glp1-oud.md
Normal file
|
|
@ -0,0 +1,34 @@
|
|||
# NCT04199728: GLP-1 Receptor Agonist for Opioid Use Disorder
|
||||
|
||||
**Type:** Clinical trial
|
||||
**Phase:** 2
|
||||
**Status:** Active (as of April 2026)
|
||||
**Intervention:** GLP-1 receptor agonist (specific drug not specified in source)
|
||||
**Target:** Opioid Use Disorder (OUD)
|
||||
|
||||
## Trial Context
|
||||
|
||||
Part of broader GLP-1 substance use disorder research program. As of April 2026, 4 OUD trials active out of 33 total SUD trials.
|
||||
|
||||
## Evidence Base
|
||||
|
||||
**Liraglutide OUD data:**
|
||||
- ~40% reduction in opioid craving in small randomized double-blind placebo-controlled residential study
|
||||
- Phase 2 evidence only
|
||||
|
||||
**Semaglutide OUD data:**
|
||||
- Significantly reduced opioid overdose risk in 1-year follow-up for patients with comorbid T2D + OUD (real-world observational data)
|
||||
- Cannot distinguish causal mechanism from selection effects
|
||||
|
||||
**Mechanism:** GLP-1 receptors in ventral tegmental area (VTA) and nucleus accumbens reduce dopamine surge from opioid exposure, attenuating reward salience.
|
||||
|
||||
**Critical limitation:** All human evidence from patients with comorbid metabolic disease. Efficacy for OUD without T2D/obesity comorbidity unknown and largely unstudied.
|
||||
|
||||
## Timeline
|
||||
|
||||
- **2026-04-28** — NBC News synthesis reports Phase 2 evidence for GLP-1 in OUD, no Phase 3 trials completed
|
||||
|
||||
## Sources
|
||||
|
||||
- NBC News/Pharmacy Times synthesis, April 2026
|
||||
- ClinicalTrials.gov NCT04199728
|
||||
|
|
@ -7,10 +7,13 @@ date: 2026-04-28
|
|||
domain: health
|
||||
secondary_domains: []
|
||||
format: news-analysis
|
||||
status: unprocessed
|
||||
status: processed
|
||||
processed_by: vida
|
||||
processed_date: 2026-05-03
|
||||
priority: medium
|
||||
tags: [GLP-1, addiction, opioid-use-disorder, nicotine, cocaine, substance-use-disorder, VTA-dopamine, reward-mechanism]
|
||||
intake_tier: research-task
|
||||
extraction_model: "anthropic/claude-sonnet-4.5"
|
||||
---
|
||||
|
||||
## Content
|
||||
Loading…
Reference in a new issue